用阿昔洛韦治疗小鼠实验性单纯疱疹性脑炎
Therapy of experimental herpes simplex encephalitis with aciclovir in mice.
作者信息
Park N H, Pavan-Langston D, McLean S L, Albert D M
出版信息
Antimicrob Agents Chemother. 1979 Jun;15(6):775-9. doi: 10.1128/AAC.15.6.775.
Abstract
This report is concerned with the capacities of aciclovir to protect mice challenged intracerebrally with multiple lethal doses of type 1 herpes simplex virus and to control multiplication of this virus in the brain. With treatment initiated 12 h after inoculation and continued for 4 consecutive days, aciclovir administered subcutaneously in daily doses ranging from 40 to 100 mg/kg led to 21-day survival rates of from 33 to 73% and reduced virus titers by 1 to (1/2) x 4 logs on postchallenge day 8. The therapeutic accomplishments of the 100-mg/kg doses of aciclovir were comparable to those of 1,000-mg/kg doses of vidarabine (9-beta-d-arabinofuranosyladenine); however, as measured by impact on body weight, aciclovir was better tolerated than vidarabine at these similarly effective doses.
摘要
本报告关注阿昔洛韦保护经脑内接种多剂致死量1型单纯疱疹病毒攻击的小鼠以及控制该病毒在脑内增殖的能力。接种后12小时开始治疗并连续进行4天,每日皮下注射剂量为40至100mg/kg的阿昔洛韦,其21天生存率为33%至73%,并在攻击后第8天将病毒滴度降低了1至(1/2)×4个对数。100mg/kg剂量的阿昔洛韦的治疗效果与1000mg/kg剂量的阿糖腺苷(9-β-D-阿拉伯呋喃糖基腺嘌呤)相当;然而,就对体重的影响而言,在这些效果相似的剂量下,阿昔洛韦比阿糖腺苷耐受性更好。
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